A Phase 3 Study of Safety and Efficacy of Karenitecin Versus Topotecan Administered for 5 Consecutive Days Every 3 Weeks in Patients With Advanced Epithelial Ovarian Cancer

The objective of this study is to assess the safety and efficacy of karenitecin versus topotecan in patients with platinum/taxane-resistant advanced epithelial ovarian cancer. Additionally, this study will assess the ability of karenitecin to extend the time to disease progression, extend the overall survival time, and reduce the incidence and severity of treatment related hematological toxicities in patients with advanced epithelial ovarian cancer.

开始日期2007-08-01

申办/合作机构

BioNumerik Pharmaceuticals, Inc.

[+1]

NCT00097903

/ Completed临床1期

Phase 1 Trial of Oral Karenitecin® in Patients With Solid Tumors"

The purpose of this study is to determine the maximum safe dose of orally administered Karenitecin (BNP1350) in patients with solid tumors.

开始日期2004-05-01

申办/合作机构

BioNumerik Pharmaceuticals, Inc.

[+1]

NCT00062491

/ Completed临床2期

Phase 2 Trial of Karenitecin (BNP1350) in Patients With Malignant Melanoma

The purpose of this study is to evaluate the safety and efficacy of Karenitecin (BNP1350) as a treatment for Malignant Melanoma.

开始日期2002-05-01

申办/合作机构

BioNumerik Pharmaceuticals, Inc.

[+1]

100 项与 Crown Bioscience International 相关的临床结果

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0 项与 Crown Bioscience International 相关的专利（医药）

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251

项与 Crown Bioscience International 相关的文献（医药）

2025-07-01·Drug Resistance Updates

MVP-LCN2 axis triggers evasion of ferroptosis to drive hepatocarcinogenesis and sorafenib resistance

Article

作者: Wu, Jun ; Wang, Qiang ; Wang, Bo ; Ma, Zhuang ; Xu, Jiawen ; Zhou, Shimeng ; Li, Mengmeng ; Zhao, Xiaoya ; Wang, Shouyu ; Ben, Jingjing ; Xu, Qingxiang ; Guo, Sheng ; Liu, Qiaoyu ; Huang, Yijin ; Wang, Zhangding ; Qian, Yun ; Shu, Chuanjun ; Chen, Chen

RNA-binding proteins (RBPs) are critical regulators in tumorigenesis and therapy resistance by modulating RNA metabolism. However, the role of RBPs in hepatocarcinogenesis and progression remains elusive. Here, RBPs screening and integrating analyses identify major vault protein (MVP) as an oncogenic RBP in the occurrence of hepatocellular carcinoma (HCC) and sorafenib resistance via suppressing ferroptosis. Mechanistically, reactive oxygen species (ROS) induces STAT3-mediated MVP transcription activation and high expression in HCC cells. Subsequently, phosphoglycerate mutase family member 5 (PGAM5) directly dephosphorylates MVP at S873, facilitating its binding to the mRNA of iron-sequestering cytokine LCN2 and maintains its stability, thereby attenuating ferroptosis by reducing lipid peroxidation and intracellular Fe²⁺ content following sorafenib treatment. Notably, tenapanor, a potent pharmacological inhibitor of MVP, effectively disrupts the interaction between MVP and LCN2 mRNA and enhances ferroptosis and sorafenib sensitivity. Collectively, these ﬁndings underscore the central role of MVP in hepatocarcinogenesis and offer promising avenues to improve HCC treatment.

2025-04-21·Cancer Research

Abstract 5195: Development of paired PDX-PDXO preclinical models for HER2-targeting ADC efficacy evaluation

作者: Zhou, Jun ; Liu, Qingzhi ; Hornsveld, Marten ; Sun, Yi ; Han, Peng ; Putker, Marrit ; Shang, Limei ; Tu, Xiaolong ; Qian, Wubin ; Zhang, Lin ; Wang, Jinxi ; Bourre, Ludovic ; Zhang, Likun ; Wang, Peng ; Wang, Jingjing ; Chen, Leilei ; Mao, Binchen

AbstractIntroduction:Tumor organoids replicate cancer lesions and capture tumor heterogeneity in vitro, and are invaluable for cancer drug development. Combining Patient-Derived Xenograft (PDX) models with corresponding Patient-Derived Xenograft Organoid (PDXO) models offers a comprehensive approach, enabling high-throughput, scalable in vitro data collection and providing insights into tumor behavior and drug responses in vivo. HER2 amplification is frequent in cancers like breast and gastric cancer, and HER2-targeted ADCs have shown exceptional efficacy. To support preclinical and mechanistic investigations that develop next-generation HER2-targeted ADCs and therapies, we established a preclinical panel of paired PDX-PDXO models with varying HER2 expression levels.Methods:Gastric (GA) and breast cancer (BR) PDXOs were generated from PDX tissue and authenticated by SNP assay. Morphology, histopathology, and genomic profiling were performed and compared with its corresponding PDX. ERBB2 expression and HER2 levels in PDX-PDXOs were detected by RNA sequencing and IHC. In vivo efficacy of 10 mpk DS8201 was studied in the PDXs, and in vitro IC50 was assessed in the PDXOs using CellTiterGlo (CTG) and High Content Imaging (HCI), allowing differentiation between cytostatic and cytotoxic responses. Correlation analysis of DS8201 response were performed based on the efficacy data from PDXOs and PDXs.Results:34 GA and 24 BR PDXOs were developed from PDX tumors originally established from patients' biopsies. Hematoxylin-eosin (H&E) staining showed distinct features within PDXOs, similar to the corresponding PDXs. High correlation (>95%) in mutation and gene expression demonstrated that PDXOs largely preserve the genomic and transcriptomic features of the originating tumors. In vivo and in vitro efficacy studies of DS8201 were performed in 14 pairs of GA and BR PDX-PDXOs, among which 12 pairs display consistent HER2 IHC scores between PDX and PDXO. Overall, 6 out of 7 DS8201-sensitive PDXOs were also sensitive in PDXs and showed tumor regression, indicating high positive predictive value (PPV: 0.857) of PDXOs. The average TGI of PDXs classified for the corresponding PDXO as sensitive is much higher than TGI of PDXs classified for the corresponding PDXO as non-sensitive (97% vs. 69%, p=0.13). Besides, DS82001 sensitivity was observed in both HER+ and HER2- models, which might relate to the bystander effect of the payload and heterogeneity of PDX.Conclusion:The paired PDX-PDXO models were successfully established and provided a novel preclinical platform for investigating mechanisms of action (MOA) and resistance in patient-relevant models matched in both in vitro and in vivo stages for developing next-generation HER2-targeting therapies.Citation Format:Jinxi Wang, Jun Zhou, Limei Shang, Qingzhi Liu, Binchen Mao, Yi Sun, Peng Han, Lin Zhang, Likun Zhang, Xiaolong Tu, Wubin Qian, Peng Wang, Leilei Chen, Marten Hornsveld, Marrit Putker, Ludovic Bourre, Jingjing Wang. Development of paired PDX-PDXO preclinical models for HER2-targeting ADC efficacy evaluation [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2025; Part 1 (Regular Abstracts); 2025 Apr 25-30; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2025;85(8_Suppl_1):Abstract nr 5195.

2025-04-21·Cancer Research

Abstract 5524: Developing KRASG12C inhibitor-resistant tumor models for efficacy evaluation of next-generation anticancer therapies

作者: Bourre, Ludovic ; Zhang, Dan ; Hua, Aaron ; Nie, Chenpan ; Feng, Jian ; Zhou, Jun ; Wang, Jessie(Jingjing) ; Wang, Peng

AbstractBackground:For decades, KRAS was considered undruggable due to the lack of suitable binding sites. However, advancements in bioengineering and chemistry have enabled the approval of targeted therapies. Success was first seen with allele-specific targeting of KRASG12C in non-small cell lung cancer (NSCLC), leading to the approval of sotorasib (AMG510, LumakrasTM). Despite its clinical benefits, resistance emerged in some patients due to secondary KRAS mutations, which necessitates next-generation or combination therapy development. In this study, we outline the development of KRASG12C inhibitor-resistant models overcome this hurdle.Methods:Secondary KRAS mutations (Y96D/C/S, H95D/Q/R, R68S, Q61H, A59T/S, and Q99L) were introduced by CRISPR/Cas9 in MIA PaCa-2 with a homozygous KRASG12C mutation. Knock-in of point mutation was validated by Sanger sequencing. Cell viability was assessed by CellTiter-Glo (CTG) with AMG510 and MRTX849 (Adagrasib, KrazatiTM). RAS-MAPK pathway activity was evaluated by western blot. Xenograft models of MIA PaCa-2 cells with Y96D/C, H95D/Q/R, R68S, Q61H and A59T were established. Additionally, in vitro chronic dosing of AMG510 generated AMG510-resistant MIA PaCa-2 and NCI-H358 cell lines were validated by CellTiter-Glo and western blot. RNA-seq identified potential resistance mechanisms. Xenograft models were also established.Results:A successful homozygous point mutation knock-in was confirmed by Sanger sequencing. Cells expressing double-mutant alleles KRAS G12C Y96D/C/S, A59T/S and R68S showed resistance to both AMG510 and MRTX849, while KRAS G12C H95D/Q/R was more resistant to MRTX849, and KRAS G12C Q61H, Q99L didn’t show significant resistance. Persistent phosphorylated ERK (pERK) and pRSK levels indicated sustained RAS-MAPK activity in cells expressing KRAS G12C Y96D, H95D, A59T/S, and R68S, even at high KRAS inhibitor concentrations. Furthermore, a KRAS G12C Y96D/C, A59T, Q61H, R68S and H95D/Q/R double mutant cell-derived xenograft was established in vivo. Additionally, MIA PaCa-2 AMG510-resistant and NCI-H358 AMG510-resistant cells showed resistance to AMG510 and MRTX849 in cell viability assays. RNA-seq data identified c-MET amplification in AMG510-resistant MIA PaCa-2 cell, while FGFR1/3/4 amplification was found in AMG510-resistant NCI-H358 cells.Conclusion:CRISPR/Cas9-engineered KRAS secondary mutations cell lines displayed differentially resistant profile to KRASG12C inhibitors, and drug-induced resistant cell models developed in vitro displayed KRAS-independent mechanisms of resistance. These novel cell models offer a valuable preclinical platform to evaluate therapeutic strategies to overcome resistance to KRAS-targeted therapies.Citation Format:Jian Feng, Dan Zhang, Aaron Hua, Chenpan Nie, Jessie(Jingjing) Wang, Ludovic Bourre, Jun Zhou, Peng Wang. Developing KRASG12C inhibitor-resistant tumor models for efficacy evaluation of next-generation anticancer therapies [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2025; Part 1 (Regular Abstracts); 2025 Apr 25-30; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2025;85(8_Suppl_1):Abstract nr 5524.

项与 Crown Bioscience International 相关的新闻（医药）

2025-02-25

·PRNewswire

Panome Bio Welcomes Jean-Pierre Wery to Its Board of Directors as it Prepares for Growth in 2025

ST. LOUIS, Feb. 25, 2025 /PRNewswire/ -- Panome Bio, a leading discovery services company, announced the addition of accomplished biotechnology leader Jean-Pierre Wery to its Board of Directors. Dr. Wery, a seasoned executive with a proven track record in scaling life sciences service companies, brings invaluable expertise to Panome Bio as it rapidly expands its operations to meet increasing customer demand. Continue Reading Panome Bio leverages metabolomics, proteomics, and multi-omic integration workflows to help biopharma discover novel biology, unravel mechanistic insights, and optimize biological systems. The company has seen substantial growth since launch in 2022, including a financing partnership with Telegraph Hill Partners and a continued expansion of their service offerings, most recently having added a suite of metabolomic tools for interrogating microbiome function. Panome Bio announces the addition of biotechnology leader Jean-Pierre Wery to its Board of Directors. Post this "We are thrilled to welcome Dr. Wery to our Board of Directors," said Edward Weinstein, CEO and Co-founder of Panome Bio. "His deep industry knowledge and strategic vision will be instrumental in guiding Panome Bio's next phase of growth. With JP's expertise, we are confident in our ability to deliver groundbreaking solutions that will transform the future of discovery sciences." Dr. Wery has substantial experience scaling CROs including as CEO of Crown Bioscience where he grew the services company to over $100M in annual revenue. "Panome Bio is at the forefront of a new era in drug discovery and clinical development," said JP Wery. "I am excited to join the Board of Directors and contribute to the company's mission of accelerating the adoption and impact of multi-omic approaches to discovery research." "JP's appointment further strengthens Panome Bio's Board of Directors and positions the company for continued success. We are confident that his leadership will drive significant value for the broader scientific community" said Deval Lashkari, Senior Partner from Telegraph Hill Partners. Deval Lashkari and his partner at Telegraph Hill, Rob Capone, are also part of Panome Bio's Board of Directors along with Edward Weinstein, and David Smoller, serial entrepreneur and Panome Bio Co-founder. About Panome Bio: Panome Bio is a contract research organization performing metabolomics, proteomics, and integrated multi-omics data analysis to help clients further their research in disease and drug development. Panome Bio provides a comprehensive workflow including experimental design, sample preparation and analysis, and data processing. For more information, please visit , follow us on LinkedIn at , or email at [email protected]. About Telegraph Hill Partners: Telegraph Hill Partners, founded in 2001 and based in San Francisco, CA, invests in commercial stage life science, medical technology, and healthcare companies. For more information, please see . Contact Information: Alexandra Harrison Director of Marketing, Panome Bio [email protected] ‪(314) 632-6588 SOURCE Panome Bio WANT YOUR COMPANY'S NEWS FEATURED ON PRNEWSWIRE.COM? 440k+ Newsrooms & Influencers 9k+ Digital Media Outlets 270k+ Journalists Opted In GET STARTED

高管变更

2024-12-11

·Business Wire

Crown Bioscience Wins 2024 Fierce CRO Award for Excellence in Client Service and Partnership

SAN DIEGO--( BUSINESS WIRE )--Crown Bioscience, a global contract research organization (CRO) headquartered in the United States and a part of JSR Life Sciences and Japan-based JSR Corporation, has been honored with the 2024 Fierce CRO Award for Excellence in Client Service and Partnership. This prestigious award recognizes Crown Bioscience's outstanding collaboration, communication, and commitment to delivering excellence for its life sciences clients. The Fierce CRO Awards, hosted annually by Fierce Biotech, celebrate the achievements of leading CROs that demonstrate innovation and leadership in accelerating drug development. Winners in this category are selected based on their commitment to building strong partnerships and providing an exceptional client experience. "Winning this award is a true testament to our team’s dedication to going above and beyond for our clients," said Dr. Jonny McMichael, Vice President of Client Experience and Enablement at Crown Bioscience. "We aim to accelerate the journey of new therapies by collaborating closely with our partners across the drug development continuum." Crown Bioscience stood out for its innovative preclinical research capabilities, transparent communication practices, and unwavering focus on delivering quality and value to clients. Specific achievements highlighted include the company's Customer Satisfaction Program , which generates unfiltered feedback scores to demonstrate its commitment to service and customer excellence. "This recognition motivates us to continue raising the bar for the CRO industry," Dr. McMichael added. "We are thankful to our entire team for making Crown Bioscience a trusted, client-focused partner in the mission to bring new treatments to patients faster and more efficiently." The full Fierce CRO Awards report profiling all winners is available here . Crown Bioscience's award-winning capabilities can be explored at www.crownbio.com . About Crown Bioscience Crown Bioscience, a JSR Life Sciences company, is a global Contract Research Organization (CRO) dedicated to improving human health through partnering with biotech and pharmaceutical companies that drive the discovery and development of oncology drugs. We exclusively offer preclinical tumor organoid services using the well-established Hubrecht Organoid Technology, with over 600 organoid models available spanning 22 cancer indications. In addition, we have developed the world’s largest commercially available PDX collection. Further committed to personalized medicine, our subsidiary, Indivumed Services, maintains an extensive biobank of liquid and tissue human biospecimens. Our focus on helping our customers develop novel therapies aims to ensure that patients receive the right treatment at the right time. Founded in 2006, we have 12 facilities across the US, Europe, and Asia. For more information, please visit www.crownbio.com

2024-08-22

·Pharmaceutical Technology

CTI announces partnership for oncology drug development

The combined expertise is expected to ensure a more effective path to clinic. Credit: Salov Evgeniy/Shutterstock. CTI Clinical Trial & Consulting Services (CTI) and Crown Bioscience have announced a strategic partnership aimed at bolstering consulting services for oncology drug development. The collaboration brings together CTI’s clinical and regulatory expertise with Crown Bioscience’s preclinical and translational models, aiming to streamline the transition of oncology compounds from discovery to early-phase global studies. It is set to benefit customers by providing expert guidance that enhances the efficiency of oncology drug development. CTI Global Laboratory Services business development vice-president Ryan Gifford stated: “Crown Bioscience’s leadership in early-phase oncology research and suite of preclinical services complement CTI’s broad spectrum of capabilities. “Together, we can offer enhanced support to our oncology clients and deepen our commitment to advancing cancer research.” See Also: FDA approves updated mRNA vaccines for Covid-19 Verve Therapeutics gets grant for gene editing compositions to lower ldl cholesterol levels The combined expertise is expected to ensure an effective path to clinic, support long-term success in drug development and accelerate the delivery of new oncology treatments to patients. Through the alliance, customers will have access to a range of consulting services designed to foster an integrated approach to drug development. These services include strategic preclinical development planning, study data analysis and interpretation, de novo assay development and regulatory guidance. Crown Bioscience commercial senior vice-president Alex Slater stated: “Crown Bioscience has an established reputation for exceeding the typical services offered by a regular CRO [contract research organisation]. “This initiative unites deep-seated expertise spanning all phases of drug development, marking a pivotal step towards delivering a true translational offer to our clients.” In November 2023, Crown Bioscience launched its service offering , OrganoidXplore to meet the demands of research initiatives by offering a diverse selection of models that cover a wide spectrum of genetic backgrounds and mutations.

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